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首页> 外文期刊>Advanced Science Letters >Enhancement of In Vitro Anti-Proliferative Activity and Intestinal Membrane Permeation of Thai Medicinal Plant Extracts Selected from the MANOSROI II Database by Loading in Chitosan-Thioglycolic Acid (TGA) Nanoparticles
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Enhancement of In Vitro Anti-Proliferative Activity and Intestinal Membrane Permeation of Thai Medicinal Plant Extracts Selected from the MANOSROI II Database by Loading in Chitosan-Thioglycolic Acid (TGA) Nanoparticles

机译:通过负载壳聚糖-巯基乙酸(TGA)纳米颗粒,从MANOSROI II数据库中选择的泰国药用植物提取物的体外抗增殖活性和肠膜渗透性增强

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Chitosan (CTS) and chitosan-thioglycolic acid (CTS-TGA) nanoparticles loaded with four aqueous extracts of Thai anti-cancer medicinal plants were prepared by ionic interaction with tripolyphosphate (TPP). The averages sizes, zeta-potentials and PDI of the CTS and CTS-TGA nanoparticles loaded with the aqueous extracts were in range of 309.09 ±66.3 to 394.6 ±71.3 nm, +1.73 ±2.39 to +2.39 ±0.79 mV and 0.354 ±0.021 to 0.555 ± 0.012; and 225.0 ±38.7 to 311.5 ±51.4 nm, 1.46 ±0.63 to 3.59 ±0.45 and 0.229 ±0.069 to 0.398 ±0.087, respectively, whereas 244.8±48.1 nm, +3.56 + 0.71 mV and 0.350; and 174.2+23.2 nm, +3.22 + 0.85 mV and 0.207, respectively were observed in blank CTS and CTS-TGA nanoparticles, respectively. All extracts from the medicinal plants showed anti-proliferative activity on HeLa and HepG2 cancer cell lines. The CTS and CTS-TGA nanoparticles can significantly enhance anti-proliferative activity of the extracts on Hela and HepG2 cancer cells (p < 0.05). The extract of T. triandra loaded in CTS nanoparticles and the extract of A. marmelos loaded in CTS-TGA nanoparticles exhibited the highest decreased cell viability of 7.28 and 6.37 folds, respectively. The in vitro kinetic release and the intestinal membrane permeation of the medicinal plant extracts determined as quinazoline through the rat intestinal membrane by Ussing type chamber across the freshly excised rat intestinal mucosa were similar to quinazoline with the release of zero order plot, whereas the release of those loaded in the CTS and CTS-TGA nanoparticles were conformed with the Higuchi's equation. Thiolation significantly enhanced the permeation of the CTS nanoparticles with the highest transport enhancement ratio (R) of 1.45 (p < 0.05). The CTS-TGA nanoparticles significantly improved the permeation of quinazoline with the highest (R) of 1.62 (p < 0.05). This study has demonstrated the anti-proliferative activity on human cancer cell lines and permeation enhancements of the Thai anti-cancer medicinal plant extracts by loading in the CTS and CTS-TGA nanoparticles, which can be further developed to oral natural products.
机译:通过与三聚磷酸酯(TPP)的离子相互作用,制备了载有泰国抗癌药用植物的四种水性提取物的壳聚糖(CTS)和壳聚糖-巯基乙酸(CTS-TGA)纳米颗粒。载有水提取物的CTS和CTS-TGA纳米颗粒的平均大小,ζ电势和PDI在309.09±66.3至394.6±71.3 nm,+ 1.73±2.39至+2.39±0.79 mV和0.354±0.021至0.555±0.012;和分别为225.0±38.7至311.5±51.4 nm,1.46±0.63至3.59±0.45和0.229±0.069至0.398±0.087,而244.8±48.1 nm,+ 3.56 + 0.71 mV和0.350;在空白的CTS和CTS-TGA纳米颗粒中分别观察到分别为174.2 + 23.2 nm,+ 3.22 + 0.85 mV和0.207。药用植物的所有提取物均对HeLa和HepG2癌细胞系具有抗增殖活性。 CTS和CTS-TGA纳米颗粒可以显着增强提取物对Hela和HepG2癌细胞的抗增殖活性(p <0.05)。负载在CTS纳米颗粒中的三叶草提取物和负载在CTS-TGA纳米颗粒中的马其菌提取物分别表现出最高的细胞活力降低,分别为7.28倍和6.37倍。用Ussing型腔室在新鲜切离的大鼠肠粘膜上通过大鼠肠膜确定的喹唑啉通过大鼠肠膜的体外动力学释放和肠膜渗透与喹唑啉相似,但释放零级图。那些装载在CTS和CTS-TGA纳米颗粒中的颗粒符合Higuchi方程。硫醇化显着增强了CTS纳米颗粒的渗透性,其最高的传输增强率(R)为1.45(p <0.05)。 CTS-TGA纳米颗粒显着改善了喹唑啉的渗透性,最高(R)为1.62(p <0.05)。这项研究表明,通过装载CTS和CTS-TGA纳米颗粒,可以对人类癌细胞系具有抗增殖活性,并增强泰国抗癌药用植物提取物的渗透性,可以将其进一步开发为口服天然产物。

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